CD38/CD31 相互作用激活导致慢性淋巴细胞白血病细胞增殖和迁移的遗传途径。
CD38/CD31 interactions activate genetic pathways leading to proliferation and migration in chronic lymphocytic leukemia cells.
机构信息
Department of Genetics, Biology and Biochemistry, of Torino Medical School, Turin, Italy.
出版信息
Mol Med. 2010 Mar;16(3-4):87-91. doi: 10.2119/molmed.2009.00146. Epub 2009 Nov 20.
Abstract
Human CD38 is a pleiotropic glycoprotein belonging to a family of enzymes/receptors involved in the catabolism of extracellular nucleotides. CD38-receptor activities are regulated through binding to the nonsubstrate ligand CD31. CD38 expression above a critical threshold is a negative prognostic marker for chronic lymphocytic leukemia (CLL) patients. Activation of CD38 by means of agonistic monoclonal antibodies or the CD31 ligand induces proliferation and immunoblast differentiation of CLL cells. Here we define the genetic signature that follows long-term in vitro interactions between CD38(+) CLL lymphocytes and CD31(+) cells. The emerging profile confirms that the CD31/CD38 axis activates genetic programs relevant for proliferative responses. It also indicates a contribution of this pathway to the processes mediating migration and homing. These results further support the notion that the CD31/CD38 axis is part of a network of accessory signals that modify the microenvironment, favoring localization of leukemic cells to growth-permissive sites.
摘要
人 CD38 是一种多功能糖蛋白,属于参与细胞外核苷酸分解代谢的酶/受体家族。CD38 受体活性通过与非底物配体 CD31 的结合来调节。CD38 的表达超过临界阈值是慢性淋巴细胞白血病 (CLL) 患者的预后不良标志物。通过激动性单克隆抗体或 CD31 配体激活 CD38 可诱导 CLL 细胞的增殖和免疫母细胞分化。在这里,我们定义了在 CD38(+) CLL 淋巴细胞与 CD31(+)细胞之间的长期体外相互作用后出现的基因特征。新兴的特征证实 CD31/CD38 轴激活了与增殖反应相关的遗传程序。它还表明该途径对介导迁移和归巢的过程有贡献。这些结果进一步支持了这样一种观点,即 CD31/CD38 轴是改变微环境的辅助信号网络的一部分,有利于白血病细胞定位到生长有利的部位。
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Highly purified CD38 sub-populations show no evidence of preferential clonal evolution despite having increased proliferative activity when compared with CD38 sub-populations derived from the same chronic lymphocytic leukaemia patient.高度纯化的CD38亚群没有显示出优先克隆进化的迹象,尽管与来自同一慢性淋巴细胞白血病患者的CD38亚群相比,其增殖活性有所增加。
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